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33 results on '"Ulla Vogel"'

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1. Acute phase response following pulmonary exposure to soluble and insoluble metal oxide nanomaterials in mice

2. The application of existing genotoxicity methodologies for grouping of nanomaterials: towards an integrated approach to testing and assessment

3. Nanomaterial- and shape-dependency of TLR2 and TLR4 mediated signaling following pulmonary exposure to carbonaceous nanomaterials in mice

4. Retained particle surface area dose drives inflammation in rat lungs following acute, subacute, and subchronic inhalation of nanomaterials

5. In vitro-in vivo correlations of pulmonary inflammogenicity and genotoxicity of MWCNT

6. Adverse outcome pathways as a tool for the design of testing strategies to support the safety assessment of emerging advanced materials at the nanoscale

7. Inhalation of welding fumes reduced sperm counts and high fat diet reduced testosterone levels; differential effects in Sprague Dawley and Brown Norway rats

8. Commentary: the chronic inhalation study in rats for assessing lung cancer risk may be better than its reputation

9. Assessment of nanomaterial-induced hepatotoxicity using a 3D human primary multi-cellular microtissue exposed repeatedly over 21 days - the suitability of the in vitro system as an in vivo surrogate

10. A response to the letter to the editor by Driscoll et al.

11. Airport emission particles: exposure characterization and toxicity following intratracheal instillation in mice

12. Health effects of exposure to diesel exhaust in diesel-powered trains

13. Effects of maternal inhalation of carbon black nanoparticles on reproductive and fertility parameters in a four-generation study of male mice

14. Maternal inhalation of carbon black nanoparticles induces neurodevelopmental changes in mouse offspring

15. Pulmonary exposure to carbonaceous nanomaterials and sperm quality

16. Primary genotoxicity in the liver following pulmonary exposure to carbon black nanoparticles in mice

17. Stat-6 signaling pathway and not Interleukin-1 mediates multi-walled carbon nanotube-induced lung fibrosis in mice: insights from an adverse outcome pathway framework

18. Editorial: dose-dependent ZnO particle-induced acute phase response in humans warrants re-evaluation of occupational exposure limits for metal oxides

19. Retained particle surface area dose drives inflammation in rat lungs following acute, subacute, and subchronic inhalation of nanomaterials

20. The application of existing genotoxicity methodologies for grouping of nanomaterials: towards an integrated approach to testing and assessment

21. A response to the letter to the editor by Driscoll et al

22. Assessment of nanomaterial-induced hepatotoxicity using a 3D human primary multi-cellular microtissue exposed repeatedly over 21 days - the suitability of the in vitro system as an in vivo surrogate

23. Primary genotoxicity in the liver following pulmonary exposure to carbon black nanoparticles in mice

24. Nano-risk Science: application of toxicogenomics in an adverse outcome pathway framework for risk assessment of multi-walled carbon nanotubes

25. Meta-analysis of transcriptomic responses as a means to identify pulmonary disease outcomes for engineered nanomaterials

26. NanoTIO2 (UV-Titan) does not induce ESTR mutations in the germline of prenatally exposed female mice

27. Carbon black nanoparticle instillation induces sustained inflammation and genotoxicity in mouse lung and liver

28. Modest effect on plaque progression and vasodilatory function in atherosclerosis-prone mice exposed to nanosized TiO(2)

29. Lung inflammation and genotoxicity following pulmonary exposure to nanoparticles in ApoE-/- mice

30. Kupffer cells are central in the removal of nanoparticles from the organism

31. Adverse outcome pathways as a tool for the design of testing strategies to support the safety assessment of emerging advanced materials at the nanoscale

32. Effects of prenatal exposure to diesel exhaust particles on postnatal development, behavior, genotoxicity and inflammation in mice

33. Distribution of silver in rats following 28 days of repeated oral exposure to silver nanoparticles or silver acetate

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